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Effects of hemocoagulase agkistrodon on the coagulation factors and its procoagulant activities

机译:血液凝结酶敏捷性对凝血因子及其促凝血活性的影响

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Objective: Hemocoagulase agkistrodon (HCA), a thrombin-like enzyme (TLE) from the venom of the Chinese moccasin snake ( Deinagkistrodon acutus ), has been used in clinical practice as a hemostatic compound. The aim of this study was to further investigate the pharmacological properties of HCA. Materials and methods: Sodium dodecyl sulfate or native polyacrylamide gel electrophoresis (SDS- or N-PAGE) as well as enzyme linked immunosorbent assays (ELISAs) were conducted to study the effects of HCA on the human plasma fibrinogen and prothrombin levels, as well as its in vitro interactions with some coagulation factors. In addition, the bleeding time effects of HCA in the mouse tail-bleeding model as well as its effects on the fibrinogen levels in rabbits were determined in vivo. Results: In vitro results revealed that HCA exerts its procoagulant activities by hydrolyzing fibrinogen into segments that are easier to be absorbed, reducing the risk of thrombus formation. Besides, HCA could significantly inhibit the activation of prothrombin at the concentration of 0.3 μM. Unexpectedly, we also found that HCA was able to strongly bind to factor X/Xa (in a ratio of 1:1) and thus inhibit the acceleration of active factor X to tissue plasminogen activator-catalyzed plasminogen activation, demonstrating that it could be less likely to lead to thrombus formation. Finally, in vivo results indicated that HCA could significantly shorten the bleeding time in the mouse tail-bleeding model and had no effect on the fibrinogen levels in rabbits. Conclusion: In summary, HCA, a unique and new family member of TLEs, may become a new clinical drug for the prevention and treatment of hemorrhage due to its unique and complex interactions with the blood system. Clarification of these features will enable us to further understand the mechanism of action of HCA and then promote its further application in clinical practice as a therapeutic drug.
机译:目的:来自中国莫卡辛蛇(Deinagkistrodon acutus)毒液的凝血酶样酶(TLE),凝血酶agkistrodon(HCA)已在临床实践中用作止血化合物。这项研究的目的是进一步研究HCA的药理特性。材料和方法:进行十二烷基硫酸钠或天然聚丙烯酰胺凝胶电泳(SDS-或N-PAGE)以及酶联免疫吸附测定(ELISA),以研究HCA对人血浆纤维蛋白原和凝血酶原水平的影响,以及它与某些凝血因子的体外相互作用。另外,在体内确定了HCA在小鼠尾巴出血模型中的出血时间效应及其对家兔纤维蛋白原水平的影响。结果:体外结果显示,HCA通过将纤维蛋白原水解成更易于吸收的片段来发挥其促凝活性,从而降低了血栓形成的风险。此外,HCA可以在0.3μM的浓度下显着抑制凝血酶原的活化。出乎意料的是,我们还发现HCA能够与因子X / Xa牢固结合(比例为1:1),从而抑制了活性因子X向组织纤溶酶原激活物催化的纤溶酶原激活的加速,表明它可能更少可能导致血栓形成。最后,体内结果表明,HCA可以显着缩短小鼠尾巴出血模型的出血时间,并且对家兔的纤维蛋白原水平没有影响。结论:总之,HCA是TLE的独特家族成员,由于其与血液系统的独特而复杂的相互作用,可能成为预防和治疗出血的新临床药物。这些特征的阐明将使我们能够进一步了解HCA的作用机理,然后促进其作为治疗药物在临床实践中的进一步应用。

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